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Targeting tumor perfusion and oxygenation to improve the outcome of anticancer therapy

机译:靶向肿瘤灌注和氧合以改善抗癌治疗的结果

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Radiotherapy and chemotherapy are widespread clinical modalities for cancer treatment. Among other biological influences, hypoxia is a main factor limiting the efficacy of radiotherapy, primarily because oxygen is involved in the stabilization of the DNA damage caused by ionizing radiations. Radiobiological hypoxia is found in regions of rodent and human tumors with a tissue oxygenation level below 10 mm Hg at which tumor cells become increasingly resistant to radiation damage. Since hypoxic tumor cells remain clonogenic, their resistance to the treatment strongly influences the therapeutic outcome of radiotherapy. There is therefore an urgent need to identify adjuvant treatment modalities aimed to increase tumor pO2 at the time of radiotherapy. Since tumor hypoxia fundamentally results from an imbalance between oxygen delivery by poorly efficient blood vessels and oxygen consumption by tumor cells with high metabolic activities, two promising approaches are those targeting vascular reactivity and tumor cell respiration. This review summarizes the current knowledge about the development and use of tumor-selective vasodilators, inhibitors of tumor cell respiration, and drugs and treatments combining both activities in the context of tumor sensitization to X-ray radiotherapy. Tumor-selective vasodilation may also be used to improve the delivery of circulating anticancer agents to tumors. Imaging tumor perfusion and oxygenation is of importance not only for the development and validation of such combination treatments, but also to determine which patients could benefit from the therapy. Numerous techniques have been developed in the preclinical setting. Hence, this review also briefly describes both magnetic resonance and non-magnetic resonance in vivo methods and compares them in terms of sensitivity, quantitative or semi-quantitative properties, temporal and spatial resolutions, as well as translational aspects.
机译:放射治疗和化疗是癌症治疗的普遍临床模式。在其他生物影响之外,缺氧是限制放射疗法疗效的主要因素,主要是因为氧涉及通过电离辐射引起的DNA损伤的稳定性。在啮齿动物和人肿瘤的区域中发现辐射生物学缺氧在10mm Hg以下的组织氧合水平,肿瘤细胞变得越来越抗辐射损伤。由于缺氧肿瘤细胞仍然是克隆语,它们对治疗的抵抗力强烈影响放射疗法的治疗结果。因此,迫切需要鉴定辅助治疗方式,旨在在放射治疗时增加肿瘤PO2。由于肿瘤缺氧从根本上引起了血管氧递送的不平衡,并且通过肿瘤细胞具有高代谢活动的肿瘤细胞的氧气消耗,因此两个有前途的方法是靶向血管反应性和肿瘤细胞呼吸的方法。本综述总结了目前关于肿瘤选择性血管扩张剂,肿瘤细胞呼吸抑制剂的知识,以及组合在肿瘤致敏中对X射线放射治疗中的所有活性的药物和治疗的知识。肿瘤选择性血管舒张也可用于改善循环抗癌剂对肿瘤的递送。成像肿瘤灌注和氧合不仅是对这种联合治疗的发展和验证的重要性,而且还可以确定哪些患者可以从治疗中受益。在临床前设置中已经开发了许多技术。因此,该综述还简要地描述了体内方法中的磁共振和非磁共振,并将它们与敏感性,定量或半定量性能,时间和空间分辨率以及平移方面进行比较。

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